Derivatives of (+)-Limonene. II. 2-Amino-1-p-menthanols1 - The

Note: In lieu of an abstract, this is the article's first page. ... Limonene Aziridines from the Commercially Available Mixture of cis- and trans-Limo...
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(2) 4-L4minobenzenesulfonylhydrazone of salicylaldehyde. Seven and five-tenths grams (0.040 mole) of 4-aminobenzenesulfonylhydrazine were dissolved in a hot solution (,omposed of 50 ml. of methanol and 50 ml. of water. To the above solution were added with stirring, 6.1 g. (0.040 mole) of salicylaldehyde. The mixture developed an orangeyellow color and became almost homogeneous. Shortly thereafter yellom-orange crystals began to precipitate from the reaction mixture. The separation of the product was facilitated by the dilution of the reaction mixture with water. The crystals were collected on a suction filter and air dried. The product weighed 11.6 g. (quantitative yield) and melted with decomposition a t 167-168'. The product was recrystallized two times from equal volumes of methanol and water. The yellow crystals weighed 5.6 g. (47y0 yield) and melted with decomposition a t 176.5177". Anal. Calcd. for C E ~ H I ~ N ~C, O 53.60; & ~ : H, 4.50; N, 14.42. Found: C, 53.71; H, 4.60; N, 14 36. (3) 4-Nitrobenzenesulfonylhydrazone of propiophenone. Seven and four-tenths grams (0.034 mole) of 4-nitrobeneenesulfonylhydrazine were dissolved in 100 ml. of hot methanol containing a little water. Four grams (0.030 mole) of propiophenone were then added dropwise with stirring. Yellow crystals separated from the reaction mixture aa it cooled to room temperature. After 2 hr. a t room temperature the crystals were collected on a suction filter and dried in a 95" oven. The yellow crystals weighed 9.8 g. (98% yield) and melted with decomposition a t 147-150'. The product was recrystallized from methanol containing a little water. The pale yellow crystals weighed 8.1 g. (817' yield) and melted with decomposition at 150-152". Anal. Calcd. for C15H15N304S: C, 54.05; H, 4.54; N, 12.61. Found: C, 54.04; H, 4.35; N, 12.41.

[CONTRIBUTION FROM

THE

(4) 4-Acetamidobenzenesulfonylhydrazcme of %cetyl-1hydroxynaphthalene. In a mortar 1.86 g. (0.01 mole) of 2-acetyl-l-hydroxynaphthalene and 2.3 g. (0.01 mole) of 4-acetamidobeneenesulfonylhydrazine were thoroughly mixed. After transferring to a large wide-diameter test tube the contents then were heated to 125" (oil bath). At this temperature the mixture liquefied somewhat and water evaporated; after 15 min., 5 ml. of glacial acetic acid and 2 drops concentrated sulfuric acid together with 15 ml. absolute ethanol were added and the mixture refluxed. After about 1 hr. everything went into Eolution. Shortly after this a yellow precipitate began to appear, after 1 additional hr. of refluxing, the contents were poured on ice, and washed with alcohol and ether. Yield 2.4 g. The compound was extremely insoluble in all common solvents. Therefore, the analytical sample was extracted with boiling alcohol. Anal. Calcd. for CZOHIQN~O~S: C, 60.44; H, 4.82; N, 10.57. Found: C, 60.23; H, 4.88; N, 10.71.

Acknowledgments. A. C. Proaay is indebted to Chattem Chemicals, a Division of the Chattanooga Medicine Company, for financial help. The authors appreciate the stimulating discussions with Drs. I. W. Grote, J. M. Holbert, and J. C. Krantz, Jr. The skillful assistance of Mr. J. E. Giesemann, H. 14. Smith, and Mrs. J. Waggoner is appreciated too. CINCINNATI 21, OHIO CHATTANOOGA 9, TEEN.

CITRUS EXPERIMENT STATION O F THE UNIVERSITY OF FLORIDA]

Derivatives of (+)-Limonene. 11. 2-Amino-l-p-menthanols' WILLIAM F. NEWHALL Received M a y 11, 1969 Several new aminoalcohols including 2-amino-l-p-menthanol have been synthesized from (+)-limonene. Partial hydrogenation of ( +)-limonene followed by oxidation with peracetic acid affords p-menthane-l,2-epoxide. The epoxide ring is readily opened hy ammonia and amines to give derivatives of 2-amino-l-p-menthanol. The direction of ring opening in p-menthane-1,2-epoxide and the configurations of the two trans isomers of 2-amino-l-p-menthanol isolated have been established by an independent synthesis from Irans-p-menthane-1,2-diolof knon-n configuration.

A number of new 2-amino-l-p-menthanols have been synthesized from (+)-limonene in connection with a study of limonene derivatives having possible physiological activity. Hydrogenation of ( +)-limonene2 without solvent, a t low pressure, over a 5% platinum on Darco G-60 catalyst proceeds smoothly to afford A'-p-menthene (I) in virtually quantitative yield. The details of this hydrogenation have been pre~ ease of sented in a previous p ~ b l i c a t i o n .This partial hydrogenation of (+)-limonene mas first

described by JTavon4and has since been utilized by a number of other authors6S6to prepare AI-pmenthene (I). Treatment of (I) with perbenzoic acid in anhydrous chloroform a t 10" according to the method of Pigulevskii and Kozhin6 affords p-menthane-l,2 epoxide (11) in 80% yield. Royals' has recently reported the preparation of (11)by hydrogenation of (+)-limonene epoxide over Adams' catalyst. Because of the difficulties inherent in the preparation of large quantities of (11) by perbenzoic acid

(1) Florida Agricultural Experiment Stations Journal Series, No. 898. (2) Samples of citrus D-limonene were supplied by Kuder Citrus Pulp Co., Lake Alfred, Fla. (3) W. F. Xewhall, J. Org. Chem., 23, 1274 (1958).

(4)hf. G. Vavon, Bull. SOC. chim. I V , 15, 282 (1914). (5) K. Fuiita and T. Matsuura, J . Sci. Hiroshima Lrniv., MA, 455 (1955). (6) G. V. Pigulevskii and S. A. Kozhin, Zhur. Obshchei Khim., 27, 803 (1957). (7) E. Earl Royals, paper no. 92, Southeastern Regional Meeting of American Chemical Society, December 1958.

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oxidation, an alternate procedure was sought employing commercially available 40% peracetic acid as the epoxidizing agent. Terry and Wheeler8 have shown that the epoxidation of natural oils can be conducted in the two-phase system which results when the oils are stirred with aqueous peracetic acid solutions. The i n situ epoxidations discussed by Gall and Greenspang were also conducted in a two-phase system maintained by using a large amount of water along with a hydrocarbon diluent. It was found that the epoxidation of (I) can be accomplished in a similar manner. The free suli'uric acid in the peracetic acid is neutralized with sodium acetate and the epoxidation performed at room temperature. Sufficient water and benzene are added to keep the reaction mixture two-phctsc at all times. Using this procedure, a 60% yield of (11) has been obtained after a reaction time of 1.5 hours. By heating at 135-140" for 24 hours in a sealed tube with excess aqueous ammonia solution, (11) is converted to a mixture of two trans aminomenthanols (111) and (IV). It is well known that the overall result of oxide formation and cleavage is equiralent to trans addition.'O Both (111) and (15') arc' represented as trans isomers of 2-amino-lp-menthanol from analogy with the work of Ropls,7 who has shown that the cleavage of (11) by ethvl alcohol under the influence of basic catalyst s yields exclusively 2-ethoxy-l-p-menthanol. Thc. configuration of (111)has been established by an independent synthesis and therefore it is reasonable to assign configuration (IV) to the other isomer isolated. The formation of (111) and (IV) is possible only if the cipoxide (11) is a mixture of isomers, one with the oxygen on the same side of the ring and the other with the oxygen on the opposite side of the ring as the isopropyl group. This is analogous to the known formation of two trans-p-menthane1,2-diols from the hydroxylation of AI-p-men(I). The mixed trans isomers of 2-methyltheiie3,lL umino-1-p-menthanol (IX), 2-dimethylamino-l-pmenthanol (X) and 2-piperidyl-l-p-menthanol (XI) are prepared in a similar manner by reaction of (11) with aqueous methylamine, aqueous dimethylz mine, and piperidine respectively. All of these aminoalcohols are high boiling, colorless, slightly viscous liquids which are strong bases only slightly soluble in water. In order to establish that the direction of cleavage of the oxide ring in (11)does proceed, as shown, to give derivatives of 1-p-menthanol, isomer (111) (8) D. E. Terry and D. H. Wheeler, U. S. Patent 2,458,484 (to Geneial ITillT, Inc.) Jan. 4, 1949. (9) R . J. Gall and F. P. Greenspan, Ind. Eng. Chem., 47, 147 (195;)). (10) Organic Chemistry, Fieser and Fieser, second ed., D. C . Heath and Company, 1950, p. 287. (11) P It. Jeffrries and B. Milligan, J. Chem. Soc., 4384 (1956).

I

y A P

A PI

II

m

y

y

A

A

HL

m

A. sla

24

.

9

of 2-amino-l-p-menthanol has been synthesized from trans-p-menthane-l,2-diol(V). The configuration of (V) is known3 from the reported work of Jefferies and Milliganll and Cole and Jefferies12 on the racemic trans-p-menthane-l,2-diols. Tertiary butyl chromate13 oxidation of (V), according to the procedure of Linder and Greenspan,14 gives the liquid keto1 (VI) which is converted by conventional means to the crystalline hydroxyoxime (VII). Hydrogenation of (VII) at low pressure over Raiiey nickel catalyst affords a mixture of the two isomers of 2-amino-l-p-menthanol (111) and (5'111) predicted from the tTyo possible orientations of the amino group. This mixture is separated by fractional crystallization of the amine picrates into two picrates, which both form crystalline hydrates. One hydrate melts at 69-73" and is converted by vacuum drying a t 85' to a crystalline, anhydrous picrate melting a t 132". The other hydrate crystallizes as yellow needles, m.p. 85-95', and is converted by vacuum drying at 64" to an amorphous glass. The aminoalcohol regenerated from this amorphous picrate is a pure, crystalline compound melting at 79.480.0". The liquid mixture of trans-2-amino-l-p-menthanols (111) and (IV) on treatment with picric acid also affords two crystalline amine picrates. One crystallizes as an anhydrous picrate melting at 187", while the other crystallizes as a hydrate (m.p. 71-74') which, on drying, affords an anhydrous picrate melting at 132". The latter picrate is identical in all respects, including infrared absorption, to the picrate melting at 132" synthesized from (V) above. (12) A. R. H. Cole and P. R. Jefferies, J . Cheni. Soc., 1391 (1956). (13) R. V. Oppenauer and H. Oberrauch, Anales asoc. quim argentim, 37, 246 (1949). (14) S. M. Tinder and F. P. Greenspan, J . Org. Chenz., 22, 949 (1957).

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This establishes the configuration of the parent aminoalcohol from the picrate melting a t 132" as (111) since the formation of (111) is predicted from each of the two reaction schemes. The aminoalcohol corresponding to the amorphous picrate (hydrate m.p. 95") must then have the configuration of (VITI). If cleavage of (11) is assumed to proceed exclusively in one direction,' (IV) must represent the configuration of the aminoalcohol from the picrate melting at 187". In contrast to the cis aminoalcohol (VIII) which, as mentioned previously, is a crystalline solid, the two trans isomers (111) and (IV) are liquids. EXPERIMENTAL

All melting points reported are uncorrected. p-Menthane-l,d-epoxide (11).Six grams of sodium acetate was added with stirring to a solution of 100 ml. of 43y0 peracetic acid (0.566 moles) in 300 ml. of water a t 25". A solution of 70 g. (0.507 moles) of A'-p-menthene ( I ) in 200 ml. of benzene was added rapidly and the resulting mixture was stirred and cooled to maintain a temperature of 22-24' for 1.5 hr. The benzene layer was then separated, washed 5 times with water, once with sodium bisulfite, once with sodium carbonate solution, and again with water until neutral. After drying over anhydrous sodium sulfate, the benzene was removed under vacuum a t 40' and the residual liquid was distilled. 4 t 69-70' (5.0 mm.) 46.8 g. (60$&) of colorless liquid was collected. This product is sufficiently pure for use directly in the preparation of 2-amino-l-pmenthanols. Redistillation to remove traces of AI-p-menthene (I) gave 42 3 g. (540j0) of p-menthane-1,2-epoxide (11), which distilled at 66.0-66.3 (5.2 mm.), n'," 1.4493; [cYJ'," $57.88 (reportedlo b.p. 66.5-66.7"/7 mm.; n'," 1.4509; [a]V +57.53). ~-Amino-l-p-menthanols(111) and (IV). Two sealed glass tubes each containing 14.5 g. of p-menthane-1,2-epoxide (11) and 24 ml. of aqueous ammonium hydroxide (28%) were heated at 135-140" for 24 hr. The cooled tubes were then opened, the contents combined and extracted once with benzene. The benzene layer was separated, dried over anhydrous sodium sulfate and the benzene removed under reduced pressure (40"). Distillation of the residual oil gave 23.2 g. ( 7 5 5 ) of I-olorless, viscous, mixed trans-2-amino1-p-menthanols (111) and (IV), b.p. 95-100' (1.5 mm.). Redistillation afforded material boiling at 100-101" (1.6 mm.). n y 1.4853, [a15 +39. Anal. Calcd. for C10H210N: C, 70.12; H, 12.36; N, 8.18. Found: C, 70.10; H, 12.18; 3 , 8.33. Twenty-four grams of the mixed trans-2-amino-l-pmenthanols (111) and (IV) (b.p. 95-100"/1.5 mm.) was fractionally distilled through an 18-inch Vigreux column a t 0.95 mm. and separated into three crude fractions. Each of the three fractions was treated with excess picric acid in methanol. After removal of the methanol under vacuum, the picrates were crystallized from water. After several recrystallizations f ram Kater, pale yellow needles, m.p. 69-73', were obtained from fraction (I). -4fter drying under vacuum at 85', thme crystals lost water of hydration and recrystallized to afford the picrate of (111),m.p. 130-132'. Anal. Calcd. for CI6&o8N4: C, 47.99; H, 6.04; N, 13.99. Found: C, 47.54; H, 5.84; N , 13.82. The free aminoalcohol (111)was not regenerated from its picrate. Yellow needles of the picrate of ( I V ) were obtained from fraction (3). After several recrystallizations from water, a sample melting a t 184-187" was obtained. -4nal. Calcd. for CL&&N(: C, 47.99; H, 6.04; N, 13.99. Found: C, 48.31; H, 5.95; h', 13.65.

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The free aminoalcohol (IV) wa.s not regenerated from its picrate. Fraction (2) contained a mixture of the two picrates isolated from fractions (1) and (3). 2-Methylamino-I-p-menthanols (IX). Reaction of p menthane-l,a-epoxide (11) with aqueous methyl amine (30%), using the same amounts of reactants and reaction conditions identical to those described for the preparation of the 2-amino-1-p-menthanols (111) and (IV), gave a liquid product which was. vacuum distilled. At 101-107' (2.0 mm.), 25.6 g. (74%) of the mixed trans isomers of 2methylamino-1-p-menthanol (IX) distilled as a colorless viscous oil. Redistillation afforded material boiling a t 9497' (1.5 mm.). n y 1.4790, [a]'," 4-44. Anal. Calcd. for Cl1H2{0N: C, 71.29; H, 12.51; N, 7.56. Found: C, 71.04; H, 12.21; K,7.59. 2-Dimethylamino-1-p-menthanols(X). Reaction of p menthane-l,2-epoxide (11) with aqueous dimethyl amine (25%), using the same amounts of reactants and reaction conditions identical to those described for the preparation of the 2-amino-1-p-menthanols (111)and (IV), gave a liquid product which was vacuum distilled. At 103-108" (2.5 mm.), 25.3 g. (68%) of the mixed trans isomers of ?-dimethylamino-1-p-menthanol (X) distilled as a colorless, fluid oil. Redistillation afforded material boiling- at 90-95 O (1.4 mm. 1. n'," 1.4722, [CY]: f36. Anal. Calcd. for CllHzsON: C, 72.30; H, 12.64; K, 7.03. Found: C. 71.81: H. 12.57: N. 6.98. 2-Piperidyl-1-p-menthanols(XI). The preparation of (XI) required more drastic conditions than that of any of the other 2-amino-1-p-menthanols. Two sealed glass tubes were prepared, each containing 14.5 g. of p-menthane-1,2epoxide (11) and 15 ml. of piperidine. This mixture is homogeneous in contrast to the two-phase systems resulting from admixture of (11) nith aqueous bases. After heating a t 145-150" for 72 hr., the cooled tubes nere opened, most of the piperidine was removed at reduced pressure (50') and the residual oil was distilled under vacuum. At 69-71" (5.1 mm.) 13.4 g. of unchanged (11) was recovered (n'," 1.4489). rZ mixture of the trans-2-piperidyl-1-p-menthanols (XI) (14.5 g.) distilled at 126-130" (1.6 mm.) as a pale yellow oil. This represents a conversion yield to (XI) of 61 %. Redistillation afforded material boiling a t 126-129" (1.6 mm.). n'," 1.4872, [CY]: +39. Anal. Calcd. for C15H290N:C, 75.25: H, 12.21, N, 5.85. Found: C, 75.67; H, 11.94; h', 5.95. 2-Keto-I-p-menthanol (VI). tert-Butyl chromate was prepared by adding 29.5 g. of chromium trioxide in small portions to 84 ml. of tert-butyl alcohol with slight cooling. A solution of 49 3 g. of trans-p-menthane-1,2-diol (I-)in 400 ml. of benzene was added dropwise to the oxidant while stirring and cooling the solution to maintain a temperature of 25-28'. The mixture was stirred for a total reaction time of 2 hr. at the same temperature. The complex was hydrolyzed by the addition in succession of 300 ml. of nater, 60 g. of hydrated oxalic acid, and 300 ml. of 2 0 5 sulfuric acid with stirring. Bfter 3 hr. the benzene layer was separated, washed once with sodium carbonate solution and dried over anhydrous sodium sulfate. After removal of the benzene at reduced pressure, the residual oil as distilled under vacuum. At 90-94" (1.4 mm.), 17.4 g. ( 3 6 5 ) of colorless, slightly viscous oil lyas collected. Redistillation afforded material boiling at 88" (1.3 mm.). n'," 1.4647, [a]'," +9.8. Anal. Calcd. for CsoH1802: C, 70.55; H, 10.66. Found: C, 69.70; H, 10.20. 2-Keto-1-p-menthanol oxime (VII). Seventeen grams of 2-keto-1-p-menthanol (VI) was warmed for a few minutes in an aqueous alcoholic solution containing 50 g. of hydroxylamine hydrochloride and 20 g. of eodium hydroxide. On cooling, colorless platelets of oxime (191)separated from solution. These crystals weighed 12.6 g. (687,) and melted a t 104-105'. Several recrystallizations from benzenepetroleum ether (30-60') solution afforded colorless prisms, [ala3 +95.69 (10% acetone solution) m.p. 105-106".

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Anal. Calcd. for C I O H I ~ O ~C,N :64.83; H, 10.34; N, 7.56. Found: C, 64.75; H, 10.50; N, 7.70. ~-Amino-l-p-menthanols(111) and (VIII). Two teaspoons of Raney nickel catalyst were added to a solution of 20 g. of (VII) in 150 ml. of methanol and hydrogenation was carried out at 50 p.s.i. at 65'. Ninety-three % of the theoretical volume of hydrogen calculated for 2 moles was taken up in 70 min. The catalyst was removed by filtration and about one half of the methanolewas evaporated from the filtratr? at reduced pressure. Excess picric acid was added together with enough water to make the solution saturated at the boiling point. A picrate crystallized from the cooled solution as yellow needles, m.p. 88-94', 22.6 g. [477&from (VII)]. This melting point was not improved after repeated recrystallizations from water. During vacuum drying a t 64', this picrate lost water of hydration and became an amorphous glass. Anal. Calcd. for ClaHzrOaNa: C, 47.99; H, 6.04; N, 13.99. Found: C, 47.47; H, 5.91; N, 13.95. The cis isomer of 2-amino-1-p-menthan01 (VIII) was re-

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generated from the hydrated picrate (m.p. 88-94') by treatment with dilute aqueous sodium hydroxide followed by ether extraction. Evaporation of the ether afforded colorless needles which were purified by vacuum sublimation. The [a]'," -97.72 sublimed material melted a t 79.4-80.0', (10% acetone solution). Anal. Calcd. for CloHzlON: C, 70.12; H, 12.36; N, 8.18. Found: C, 69.85; H, 11.86; N, 8.26. The filtrate from the above picrate (m.p. 88-94') wm evaporated to dryness under vacuum and the residue dissolved in water. A crystalline picrate m.p. 63-72' (10.4 g.) [21.770 from (VII)] separated slowly from the cooled solution. Several recrystallizations from --ater afforded pale yellow needles, m.p. 71-74'. After drying under vacuum at 85', these crystals lost water of hydration and recrystallized to give the picrate of 111, m.p. 130-132". A mixture of this picrate with the picrate (m.p. 130-132") prepared from (11) showed no melting point depression. LAKEALFRED,FLA.

ORGANIC CHEMICALS DIVISION,ST. Lours RESEARCH DEPARTMENT, MONSANTO CHEMICAL ] COMPANY

The Preparation and Bacteriostatic Activity of Substituted rn-Ni trocarbanilides D. J. BE.4VER, D. P. R0;\1.4N,

AND

P. J. STOFFEL

Received May 20, 1959 The preparation and in vitro bacteriostatic activity of some substituted m-nitrocarbanilides against Staphylococms aureus are described. A discussion of specific activity as related t o chemical structiire is included.

The present paper is a continuation of work described previously1V2interrelating chemical structure with bacteriostatic activity. The remarkable specificity encountered in the tri- and tetra-chlorocarbanilides3 has now been duplicated in the substituted nitrocarbanilides. I n both cases, antimicrobial activity mas enhanced or completely loet with slight modifications in chemical structure. The more effective nitrocarbanilides completely inhibited the growth of Staphylococcus aureus (SA) in dilutions of one to ten million. I n the course of screening the carbanilides reported in this paper it was soon apparent that the substituted nitrocarbanilides were as specific iii their structural requirements to obtain bacteriostatic activity as was found previously for the trichlor~carbanilides.~ The 3-nitrocarbanilides were found to be inactive unless substituted wit,h a halogen in the 3 position of the second phenyl ring when the maximum activity a t a dilution of one part to ten million parts was obtained. The presence of either the nitro or the halogen in positions other than the 3 position completely inactivated the com(1) D. J. Beaver and P. J. Stoffel, J . Am. Chem. SOC.,

74, 3410 (1952). ( 2 ) D. J. Beaver, R. S. Shumard, a n d P . J. Stoffel, J . Am. Chem. Soc., 75,5579 (1953). (3) D. J. Beaver, D. P. Roman, and P. J. Stoffel, J. Am. Chem. SOC.,79, 1236 (1957).

pounds. These data are shown in groups A and B. (The compounds are numbered consecutively for ready cross reference to Table I where their physical properties are listed) GROUPA

SO.

R

R

4

Chloro Kitro Xitro

Chloro Sitro Chloro

8 6

SL44

j

0 0 10 Million

GROUPB

SO.

R

24 5 23 35

2-Nitro 2-Nitro 3-Sitro 3-h'i tro 3-Nitro 4-Nitro 4Nitro 2-Kitro

7 34 1 2

SA 2-Nitro 4-Chloro 2-Nitro 2-Methyl-5-nitro PChloro 4-Nitro 3-CDichloro 3.4-Dichloro

(4) In groups A-F, the figures under "SA" refer to the maximum dilution which will completely inhibit the growth in vitro of the organism Staphylococcus auras. The bacteriostatic test procedure is described in ref. (3).